[HTML][HTML] The mitogen and stress-activated protein kinase 1 regulates the rapid epigenetic tagging of dorsal horn neurons and nocifensive behaviour
KK Tochiki, M Maiarú, C Norris, SP Hunt, SM Géranton - Pain, 2016 - journals.lww.com
KK Tochiki, M Maiarú, C Norris, SP Hunt, SM Géranton
Pain, 2016•journals.lww.comPhosphorylation of histone H3 at serine 10 (p-H3S10) is a marker of active gene
transcription. Using cognitive models of neural plasticity, p-H3S10 was shown to be
downstream of extracellular signal-regulated kinase (ERK) signalling in the hippocampus. In
this study, we show that nociceptive signalling after peripheral formalin injection increased p-
H3S10 expression in the ipsilateral dorsal horn. This increase was maximal 30 minutes after
formalin injection and occurred mainly within p-ERK-positive neurons. Spinal p-H3S10 …
transcription. Using cognitive models of neural plasticity, p-H3S10 was shown to be
downstream of extracellular signal-regulated kinase (ERK) signalling in the hippocampus. In
this study, we show that nociceptive signalling after peripheral formalin injection increased p-
H3S10 expression in the ipsilateral dorsal horn. This increase was maximal 30 minutes after
formalin injection and occurred mainly within p-ERK-positive neurons. Spinal p-H3S10 …
Abstract
Phosphorylation of histone H3 at serine 10 (p-H3S10) is a marker of active gene transcription. Using cognitive models of neural plasticity, p-H3S10 was shown to be downstream of extracellular signal-regulated kinase (ERK) signalling in the hippocampus. In this study, we show that nociceptive signalling after peripheral formalin injection increased p-H3S10 expression in the ipsilateral dorsal horn. This increase was maximal 30 minutes after formalin injection and occurred mainly within p-ERK-positive neurons. Spinal p-H3S10-enhanced expression was also observed in neurokinin 1 receptor (NK1R), c-Fos, and Zif268 positive neurons and was inhibited by ablation of serotonergic descending controls. The mitogen and stress-activated protein kinase 1 (MSK1) is downstream of ERK and can induce p-H3S10. We found that, after formalin injection, most phospho-MSK1 (p-MSK1)-positive cells (87% 6 3%) expressed p-ERK and the majority of p-H3S10-positive cells (85% 6 5%) expressed p-MSK1. Inhibition of ERK activity with the MEK inhibitor SL327 reduced formalin-induced p-ERK, p-MSK1, and p-H3S10, demonstrating that spinal p-MSK1 and p-H3S10 were at least partly downstream of ERK signalling. Crucially, pharmacological blockade of spinal MSK1 activity with the novel MSK1 inhibitor SB727651A inhibited formalin-induced spinal p-H3S10 and nocifensive behaviour. These findings are the first to establish the involvement of p-H3S10 and its main kinase, MSK1, in ERK regulation of nociception. Given the general importance of ERK signalling in pain processing, our results suggest that p-H3S10 could play a role in the response to injury.
Lippincott Williams & Wilkins
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